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Paul Bollyky

Academic Appointments

Key Documents

Contact Information

  • Academic Offices
    Personal Information
    Email Tel (650) 723-7823

Professional Overview

Honors and Awards

  • Elected to membership, Western Society of Clinical Investigators (2012)
  • Young Investigator Award, University of Washington Diabetes Research Council (2012)
  • Career Development Award, Juvenile Diabetes Research Foundation (2012)
  • Genentech/Biogen Travel Award, FOCIS conference (2009)
  • Trainee Presentation Award, Federation of Clinical Immunology Societies (FOCIS) (2008)
  • K08 Mentored Clinical Scientist Award, NIH/NIAID ((2007-2012))
View All 14honors and awards of Paul Bollyky

Professional Education

Board Certification: American Board of Internal Medicine, Infectious Diseases (2007)
Board Certification: American Board of Internal Medicine, Internal Medicine (2004)
Fellowship: University of Washington, Infectious Diseases (2007)
Residency: Brigham and Women's Hospital, Internal Medicine (2004)
M.D.: Harvard Medical School, Medicine (2001)
D.Phil: Oxford University, Zoology (1998)
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Postdoctoral Advisees

Shannon Ruppert

Graduate & Fellowship Program Affiliations

Scientific Focus

Current Research Interests

Our lab studies the extracellular matrix (ECM) and it's role in the immune response to injury and infection. Our goals are 1. to understand how inflammation drives immune dysregulation, such as that seen in asthma, autoimmunity and chronic infections and 2. to devise novel strategies and tools to promote immune tolerance.

In one set of studies, we are investigating the immunologic properties of hyaluronan (HA) a long polysaccharide produced in copious amounts in inflamed tissues. Our hypothesis is that the size of HA provides contextual cues that govern immune regulation in injured and healing tissues. We and others have reported that high molecular weight hyaluronan (HMW-HA), typical of healing tissues, is anti-inflammatory via its interactions with CD44. In contrast. low molecular weight HA (LMW-HA), generated from HA catabolism at sites of active inflammation, is pro-inflammatory and an agonist of Toll-like receptors (TLR). We are funded to examine the cellular machinery underlying these interactions. Specifically, we are investigating the cross-regulation of CD44 and TLR signaling and how HA size impacts the function and number of FoxP3+ regulatory T-cells. We want to know whether strategies to promote ECM integrity in vivo can be used to prevent immune dysregulation in mouse models of autoimmune diabetes and asthma and whether bioengineered matrices can recapitulate tissue integrity signals and promote immune tolerance.

In a second set of studies, we are examining how the matrix produced by microbial pathogens modulates host immune responses. Our hypothesis is that capsular polysaccharides and biofilms influence leukocyte behavior in ways that are similar to how HA does in healing tissues. We want to know how these structures promote chronic infections and whether we can mine them for biomaterials to promote immune tolerance.

We welcome both graduate students and post-doctoral fellows, particularly individuals with interests in either matrix biology,, biochemistry, immunology or bioengineering.

Publications

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